Nature Communications (Oct 2024)

Direct recognition of an intact foreign protein by an αβ T cell receptor

  • Catarina F. Almeida,
  • Benjamin S. Gully,
  • Claerwen M. Jones,
  • Lukasz Kedzierski,
  • Sachith D. Gunasinghe,
  • Michael T. Rice,
  • Richard Berry,
  • Nicholas A. Gherardin,
  • Trang T. Nguyen,
  • Yee-Foong Mok,
  • Josephine F. Reijneveld,
  • D. Branch Moody,
  • Ildiko Van Rhijn,
  • Nicole L. La Gruta,
  • Adam P. Uldrich,
  • Jamie Rossjohn,
  • Dale I. Godfrey

DOI
https://doi.org/10.1038/s41467-024-51897-3
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 18

Abstract

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Abstract αβ T cell receptors (αβTCRs) co-recognise antigens when bound to Major Histocompatibility Complex (MHC) or MHC class I-like molecules. Additionally, some αβTCRs can bind non-MHC molecules, but how much intact antigen reactivities are achieved remains unknown. Here, we identify an αβ T cell clone that directly recognises the intact foreign protein, R-phycoerythrin (PE), a multimeric (αβ)6γ protein complex. This direct αβTCR–PE interaction occurs in an MHC-independent manner, yet triggers T cell activation and bound PE with an affinity comparable to αβTCR–peptide–MHC interactions. The crystal structure reveals how six αβTCR molecules simultaneously engage the PE hexamer, mediated by the complementarity-determining regions (CDRs) of the αβTCR. Here, the αβTCR mainly binds to two α-helices of the globin fold in the PE α-subunit, which is analogous to the antigen-binding platform of the MHC molecule. Using retrogenic mice expressing this TCR, we show that it supports intrathymic T cell development, maturation, and exit into the periphery as mature CD4/CD8 double negative (DN) T cells with TCR-mediated functional capacity. Accordingly, we show how an αβTCR can recognise an intact foreign protein in an antibody-like manner.